Hepatotoxicity and nephrotoxicity of 3-bromopyruvate in mice

Fifteen nude mice were grafted subcutaneously in the left flank with MDA-MB-231 cells, then all mice were divided into control group (PBS), 3BP group (8 mg/kg), positive group (DNR: 0.8 mg/kg) when tumor volume reached approximately 100 mm³. 28 days later, tumors, livers and kidneys were stored in 4 % formalin solution and stained with hematoxylin and eosin staining. The Kunming mice experiment included control group (PBS), 3BP group (4mg/kg; 8mg/kg; 16mg/kg), positive group (DNR: 0.8 mg/kg). 24 hours later, the blood were used for the determination of hepatic damage serum biomarkers. Livers were stored in 4 % formalin solution for the later detection.

RESULTS:

3BP at the dose of 8mg/kg had a good effect on inhibiting tumor growth in nude mice and did not damage liver and kidney tissues. Kunming mice experiment showed 3BP at the dose of 16mg/kg did damage to liver tissues.

CONCLUSION:

3-Bromopyruvate at the dose of suppressing tumor growth did not exhibit hepatotoxicity and nephrotoxicity in nude mice, and the effect on liver was confirmed in Kunming mice.

Key words:
Bromopyruvate; Hepatotoxicity; Nephrotoxicity; Mice

Authorship

Qiong Pan

Graduate student, Department of Pharmacy, China. Technical procedures, manuscript preparation.Department of PharmacyChinaChinaGraduate student, Department of Pharmacy, China. Technical procedures, manuscript preparation.

Yiming Sun

Graduate student, Department of Pharmacy, China. Technical procedures.Department of PharmacyChinaChinaGraduate student, Department of Pharmacy, China. Technical procedures.

Qili Jin

Assistant Professor, Department of Pathology, China. Technical procedures.Department of PathologyChinaChinaAssistant Professor, Department of Pathology, China. Technical procedures.

Qixiang Li

Graduate student, Department of Pharmacy, China, Technical procedures.Department of PharmacyChinaChinaGraduate student, Department of Pharmacy, China, Technical procedures.

Qing Wang

Assistant Professor, Department of Pharmacy, China. Conception and design of the study, critical revision.Department of PharmacyChinaChinaAssistant Professor, Department of Pharmacy, China. Conception and design of the study, critical revision.

Hao Liu

Full Professor, Department of Pharmacy, China. Conception and design of the study.Department of PharmacyChinaChinaFull Professor, Department of Pharmacy, China. Conception and design of the study.

Surong Zhao

Correspondence: Hao Liu Bengbu Medical College, Anhui - China Phone: +865523175230 Fax: +865523175234 liuhao6886@foxmail.com

Conflict of interest:

none

SCIMAGO INSTITUTIONS RANKINGS

Graduate student, Department of Pharmacy, China. Technical procedures.Department of PharmacyChinaChinaGraduate student, Department of Pharmacy, China. Technical procedures.

Assistant Professor, Department of Pathology, China. Technical procedures.Department of PathologyChinaChinaAssistant Professor, Department of Pathology, China. Technical procedures.

Graduate student, Department of Pharmacy, China, Technical procedures.Department of PharmacyChinaChinaGraduate student, Department of Pharmacy, China, Technical procedures.

Full Professor, Department of Pharmacy, China. Conception and design of the study.Department of PharmacyChinaChinaFull Professor, Department of Pharmacy, China. Conception and design of the study.

Figures

Figures (3)

Thumbnail

FIGURE 1
Antitumor effect of 3BP in nude mice. Breast cancer cells MDA-MB-231 were inoculated subcutaneously to induce tumor formation. Mice with tumors (100mm³3 Pedersen PL. 3-Bromopyruvate (3BP) a fast acting, promising, powerful, specific, and effective "small molecule" anti-cancer agent taken from labside to bedside: introduction to a special issue. J Bioenerg Biomembr. 2012;44(1):1-6. PMID: 22382780.) were randomly divided into three groups (5 mice/group). The tumor volume was calculated from day 8. a. Comparison of tumor volumes. Tumor growth was monitored every 4 days and calculated with the formula: length x width²2 Xian SL, Cao W, Zhang XD, Lu YF. 3-Bromopyruvate inhibits human gastric cancer tumor growth in nude mice via the inhibition of glycolysis. Oncology Letters. 2015;9(2):739-44. PMID: 25621044./2. b. Comparison of the transplanted tumor. Tumors were quickly removed after animals were sacrificed, take a photograph of them for comparison. c. H&E staining of tumor tissues in vivo. 3BP at 16mg/kg caused part of necrosis tumor issues compared with the control group.

Thumbnail

FIGURE 2
The effect of 3BP on liver and kidney in nude mice. The analysis of blood chemistry indicator. The blood was collected from animal eyes. The samples of blood were stewing for half an hour, taking the upper serum after centrifugation (1500 r/m, 10 min), then analyzed by automatic biochemical analyzer. a. The analysis of the activity of AKP, ALT and AST in serum changed indistinctively in drug groups compared with the control group (p>0.05). b. H&E staining of liver tissues in vivo. 3BP at 8mg/kg caused no hepatotoxicity compared with the control group. c. The concentration of BUN, UA and CER in serum changed indistinctively (p>0.05). d. H&E staining of kidney tissues in vivo. 3BP at 8mg/kg caused no nephrotoxicity compared with the control group.

Thumbnail

FIGURE 3
The effect of 3BP on liver in Kunming mice. a. Comparison of liver index. Liver was collected after animals were sacrificed and were calculated with the formula: liver index weight/body weight×100%. Liver index in 3BP (4mg/kg) group were higher compared with the control group (p>0.05). With the increasing drug dose, the liver index in 3BP (8mg/kg) group and 3BP (16mg/kg) group was almost equal. b. Comparison of activity of ALT and AST in serum increased in drug groups, 3BP at 4 mg/kg and 8mg/kg did not change significantly compared with the control group (p>0.05), while 3BP at 16mg/kg group changed significantly (p<0.05). c. H&E staining of liver tissues in vivo. 3BP at 4mg/kg and 8mg/kg did not cause hepatotoxicity compared with the control group. d. The effect of 3BP on expression of GAPDH in liver. The expression level of GAPDH at 4mg/kg 3BP and 8mg/kg 3BP group changed fairly compared with control group. e. The effect of 3BP on apoptosis. There were few apoptotic cells in 3BP at 4mg/kg and 8mg/kg group, while 16mg/kg group were changed significantly compared with the control group.

FIGURE 1 Antitumor effect of 3BP in nude mice. Breast cancer cells MDA-MB-231 were inoculated subcutaneously to induce tumor formation. Mice with tumors (100mm³3 Pedersen PL. 3-Bromopyruvate (3BP) a fast acting, promising, powerful, specific, and effective "small molecule" anti-cancer agent taken from labside to bedside: introduction to a special issue. J Bioenerg Biomembr. 2012;44(1):1-6. PMID: 22382780.) were randomly divided into three groups (5 mice/group). The tumor volume was calculated from day 8. a. Comparison of tumor volumes. Tumor growth was monitored every 4 days and calculated with the formula: length x width²2 Xian SL, Cao W, Zhang XD, Lu YF. 3-Bromopyruvate inhibits human gastric cancer tumor growth in nude mice via the inhibition of glycolysis. Oncology Letters. 2015;9(2):739-44. PMID: 25621044./2. b. Comparison of the transplanted tumor. Tumors were quickly removed after animals were sacrificed, take a photograph of them for comparison. c. H&E staining of tumor tissues in vivo. 3BP at 16mg/kg caused part of necrosis tumor issues compared with the control group.

FIGURE 2 The effect of 3BP on liver and kidney in nude mice. The analysis of blood chemistry indicator. The blood was collected from animal eyes. The samples of blood were stewing for half an hour, taking the upper serum after centrifugation (1500 r/m, 10 min), then analyzed by automatic biochemical analyzer. a. The analysis of the activity of AKP, ALT and AST in serum changed indistinctively in drug groups compared with the control group (p>0.05). b. H&E staining of liver tissues in vivo. 3BP at 8mg/kg caused no hepatotoxicity compared with the control group. c. The concentration of BUN, UA and CER in serum changed indistinctively (p>0.05). d. H&E staining of kidney tissues in vivo. 3BP at 8mg/kg caused no nephrotoxicity compared with the control group.

FIGURE 3 The effect of 3BP on liver in Kunming mice. a. Comparison of liver index. Liver was collected after animals were sacrificed and were calculated with the formula: liver index weight/body weight×100%. Liver index in 3BP (4mg/kg) group were higher compared with the control group (p>0.05). With the increasing drug dose, the liver index in 3BP (8mg/kg) group and 3BP (16mg/kg) group was almost equal. b. Comparison of activity of ALT and AST in serum increased in drug groups, 3BP at 4 mg/kg and 8mg/kg did not change significantly compared with the control group (p>0.05), while 3BP at 16mg/kg group changed significantly (p<0.05). c. H&E staining of liver tissues in vivo. 3BP at 4mg/kg and 8mg/kg did not cause hepatotoxicity compared with the control group. d. The effect of 3BP on expression of GAPDH in liver. The expression level of GAPDH at 4mg/kg 3BP and 8mg/kg 3BP group changed fairly compared with control group. e. The effect of 3BP on apoptosis. There were few apoptotic cells in 3BP at 4mg/kg and 8mg/kg group, while 16mg/kg group were changed significantly compared with the control group.

How to cite

copy

Sociedade Brasileira para o Desenvolvimento da Pesquisa em Cirurgia https://actacirbras.com.br/ - São Paulo - SP - Brazil
E-mail: actacirbras@gmail.com

Acompanhe os números deste periódico no seu leitor de RSS

Versão para download de PDF

PDF

Inglês

Versões e tradução automática

Versão original do texto

English

Tradução automática

Google Translator
Microsoft Translator

Como citar

RIS

BIBTEX

Outros formatos de citação e exportação:

SciELO - Scientific Electronic Library Online
Rua Dr. Diogo de Faria, 1087 – 9º andar – Vila Clementino 04037-003 São Paulo/SP - Brasil
E-mail: scielo@scielo.org